A　series　of　novel　morpholin-3-one-fused　quinazoline　derivatives　were　designed,　synthesized　and　evaluated　as　EGFR　tyrosine　kinase　inhibitors.　Nineteen　compounds　showed　significant　inhibitory　activities　against　EGFR(wt)　kinase　(IC50　＜　1　mu　M).　Compound　a8　demonstrated　the　most　potent　inhibitory　activity　toward　EGFRwt　(IC50　=　53.1　nM).　Compound　a7　and　a8　showed　excellent　inhibitory　activities　against　mutant　EGFR(T790M/L858R)　and　strong　antiproliferative　activity　against　H358　and　A549　cell　lines.　Finally,　molecular　docking　studies　were　performed　to　predict　the　possible　binding　mode　of　the　target　compounds.　It　is　believed　that　this　work　would　be　very　useful　for　designing　a　new　series　of　tyrosine　kinase　inhibitors　targeting　EGFR.　(C)　2016　Published　by　Elsevier　Ltd.